Literature DB >> 15381761

Random mutagenesis and selection of Escherichia coli cytosine deaminase for cancer gene therapy.

Sheri D Mahan1, Greg C Ireton, Catherine Knoeber, Barry L Stoddard, Margaret E Black.   

Abstract

Cytosine deaminase (CD) is currently being used as a suicide gene for cancer gene therapy. The premise of this therapy is the preferential deamination of 5-fluorocytosine (5FC) to 5-fluorouracil by cancer cells expressing cytosine deaminase. However, a lack of efficient gene transfer to tumors combined with inefficient 5FC turnover currently limits the clinical applications of this gene therapy approach. We have used random mutagenesis to create novel bacterial cytosine deaminases that demonstrate an increased preference for 5FC over cytosine. Among the 15 mutants isolated, one conferred sensitivity to Escherichia coli in a negative selection system at a concentration of 5FC that was 10-fold lower than a sublethal dose for wild-type CD. Evaluation of individual substitutions found in this double mutant (Q102R, D314G) demonstrated that the substitution at residue D314 was solely responsible for the observed increase in sensitivity to 5FC. Additional mutagenesis at D314 resulted in the identification of two more substitutions with the ability to confer enhanced 5FC sensitivity to E.coli. Structure determinations of the three CD variants in the presence and absence of a transition state 5FC analogue provide insights to the determinants of substrate binding specificity at the 5' position of the pyrimidine ring. CD mutant D314A is a promising candidate for further gene therapy studies.

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Year:  2004        PMID: 15381761     DOI: 10.1093/protein/gzh074

Source DB:  PubMed          Journal:  Protein Eng Des Sel        ISSN: 1741-0126            Impact factor:   1.650


  22 in total

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2.  Use of adenoviral vectors to target chemotherapy to tumor vascular endothelial cells suppresses growth of breast cancer and melanoma.

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4.  Antitumor activity of mutant bacterial cytosine deaminase gene for colon cancer.

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Journal:  World J Gastroenterol       Date:  2011-06-28       Impact factor: 5.742

Review 5.  Enzymes to die for: exploiting nucleotide metabolizing enzymes for cancer gene therapy.

Authors:  Andressa Ardiani; Adam J Johnson; Hongmei Ruan; Marilyn Sanchez-Bonilla; Kinta Serve; Margaret E Black
Journal:  Curr Gene Ther       Date:  2012-04-01       Impact factor: 4.391

Review 6.  Chapter seven--Cancer treatment with gene therapy and radiation therapy.

Authors:  Sergey A Kaliberov; Donald J Buchsbaum
Journal:  Adv Cancer Res       Date:  2012       Impact factor: 6.242

7.  Computational Design of a Photocontrolled Cytosine Deaminase.

Authors:  Kristin M Blacklock; Brahm J Yachnin; G Andrew Woolley; Sagar D Khare
Journal:  J Am Chem Soc       Date:  2017-12-28       Impact factor: 15.419

8.  Monitoring enzyme activity using a diamagnetic chemical exchange saturation transfer magnetic resonance imaging contrast agent.

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Journal:  J Am Chem Soc       Date:  2011-09-23       Impact factor: 15.419

9.  n-->pi* interactions in proteins.

Authors:  Gail J Bartlett; Amit Choudhary; Ronald T Raines; Derek N Woolfson
Journal:  Nat Chem Biol       Date:  2010-07-11       Impact factor: 15.040

10.  A general life-death selection strategy for dissecting protein functions.

Authors:  Po Hien Ear; Stephen W Michnick
Journal:  Nat Methods       Date:  2009-10-11       Impact factor: 28.547

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